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Neuroprotective effect of small heat shock protein, Hsp27, after acute and chronic alcohol administration

机译:小剂量热休克蛋白Hsp27在急慢性酒精中的神经保护作用

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Alcohol induces degeneration of neurons and inhibits neurogenesis in the brain. Small heat shock proteins are able to protect neurons in cerebral ischemia and oxidative stress. In this study, we investigated the neuroprotective effect of small heat shock protein, Hsp27, after acute and chronic ethanol administrations using transgenic mice overexpressing the human Hsp27 protein. Transgenic mice and wild-type littermates were injected with 2 g/kg ethanol intraperitoneally, and then motor coordination and muscle strength were analyzed using different behavioral tests, such as footprint analysis, balance beam, and inverted screen tests. Ethanol-injected transgenic mice showed similar footprints to control saline-injected mice, did not fall of the beam, and were able to climb to the top of the inverted screen, while wild-type mice showed ataxia and incoordination after ethanol injection. The effect of Hsp27 on chronic ethanol consumption was also investigated. Drinking water of mice was replaced by a 20% ethanol solution for 5 weeks, and then brain sections were stained with Fluoro Jade C staining. We found significantly lesser amount of degenerating neurons in the brain of ethanol-drinking transgenic mice compared to wild-type mice. We conclude that Hsp27 can protect neurons against the acute and chronic toxic effects of ethanol.
机译:酒精会诱导神经元变性并抑制大脑中的神经发生。小型热激蛋白能够保护脑缺血和氧化应激中的神经元。在这项研究中,我们使用过表达人类Hsp27蛋白的转基因小鼠在急性和慢性乙醇给药后研究了小热休克蛋白Hsp27的神经保护作用。向转基因小鼠和野生型同窝小鼠腹膜内注射2 g / kg乙醇,然后使用不同的行为测试(例如足迹分析,平衡木和倒置屏幕测试)分析运动协调和肌肉力量。注射乙醇的转基因小鼠显示出与对照注射盐水的小鼠相似的足迹,没有落下光束,并且能够爬到倒置屏幕的顶部,而野生型小鼠在注射乙醇后表现出共济失调和不协调。还研究了Hsp27对慢性乙醇消耗的影响。用20%乙醇溶液代替小鼠的饮用水5周,然后用Fluoro Jade C染色对脑切片进行染色。我们发现,与野生型小鼠相比,喝乙醇的转基因小鼠的大脑中退化神经元的数量要少得多。我们得出的结论是,Hsp27可以保护神经元免受乙醇的急性和慢性毒性作用。

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